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首页> 外文期刊>Brain research >Increasing proportions of tyrosine hydroxylase-immunoreactive intemeurons colocalize with choline acetyltransferase or vasoactive intestinal peptide in the developing rat cerebral cortex
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Increasing proportions of tyrosine hydroxylase-immunoreactive intemeurons colocalize with choline acetyltransferase or vasoactive intestinal peptide in the developing rat cerebral cortex

机译:在发育中的大鼠大脑皮层中,酪氨酸羟化酶免疫反应性内胚层与胆碱乙酰转移酶或血管活性肠肽共定位的比例增加

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摘要

Cortical intemeurons are critical for information processing, and their dysfunction has been implicated in neurological disorders. One subset of this diverse cell population expresses tyrosine hydroxylase (TH) during postnatal rat development Cortical TH-immunoreactive neurons appear at postnatal day (P) 16. The number of TH cells sharply increases between P16 and P20 and subsequently decreases to adult values. The absence of apoptotic markers in these cells suggests that the reduction in cell number is not due to cell death but is due to a decline in TH production. Cortical TH cells lack all additional catecholaminergic enzymes, and many coexpress GABA and calretinin, but little else is known about their phenotype or function. Because intemeurons containing choline acetyltransferase (ChAT) or vasoactive intestinal peptide (VIP) share characteristics with cortical TH neurons, the coexpression of TH with ChAT or VIP was examined throughout the neocortex at P16, P20, and P30. The proportions of TH cell profiles double-labeled for ChAT or VIP significantly increased between P16 and P30. Based on their proximity to blood vessels, intrinsic cholinergic and VIPergic cells have been hypothesized to regulate cortical microdrculation. Labeling with the gliovascular marker aquaporin-4 revealed that at least half of the TH cells were apposed to microvessels at these ages, and many of these cells contained ChAT or VIP. Cortical TH neurons did not coproduce nitric oxide synthase. These results suggest that increasing proportions of cortical TH neurons express ChAT or VIP developmentally and that a subset of these TH neurons may regulate local blood flow.
机译:皮质间质对于信息处理至关重要,其功能障碍与神经系统疾病有关。这种多样化的细胞群中有一个亚群在出生后的大鼠发育过程中表达酪氨酸羟化酶(TH)。皮质TH免疫反应性神经元出现在出生后的第16天。在P16和P20之间,TH细胞的数量急剧增加,随后减少到成年。这些细胞中不存在凋亡标记,这表明细胞数量的减少不是由于细胞死亡,而是由于TH产生的下降。皮质TH细胞缺乏所有其他儿茶酚胺能酶,并且许多共表达GABA和钙调蛋白,但对其表型或功能知之甚少。由于含有胆碱乙酰基转移酶(ChAT)或血管活性肠肽(VIP)的内胚层与皮质TH神经元具有共同的特征,因此在整个新皮层的P16,P20和P30都检查了TH与ChAT或VIP的共表达。在P16和P30之间,双标记ChAT或VIP的TH细胞谱的比例显着增加。根据它们与血管的接近程度,已假设内在的胆碱能和VIPergic细胞可调节皮层微调。用脑血管标记aquaporin-4进行标记显示,在这些年龄,至少一半的TH细胞与微血管并置,其中许多细胞都含有ChAT或VIP。皮质TH神经元不共同产生一氧化氮合酶。这些结果表明,越来越多的皮质TH神经元表达ChAT或VIP,并且这些TH神经元的一部分可以调节局部血流。

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